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T h e H i s t o r y a n dD e v e l o p m e n t o f t h e

GastroenteropancreaticE n d o c r i n e A x i s

Eric H. Liu, MDa, Kjell Oberg, MD, PhDb,*

The history of the gastroenteropancreatic (GEP) endocrine axis is a rich heritage filled

with glorious stories of triumphant discoveries and miracle cures. However, it is also

filled with drama, clash of egos and personalities, and reformulations of previous

dogma. While scientists slowly developed new concepts of a diffuse neuroendocrine

system, at the center of these stories were patients suffering from mysterious

syndromes and childhood death. A few historic names in the field of medicine includeBayliss, Starling, Banting, Kocher, Whipple, and Cushing; their work has been honored

by numerous Nobel prizes and immortalized in the medical language spoken by gener-

ations of physicians and scientists. Through their work, a mature concept of the endo-

crine system has emerged not only in the traditional secretory organs, but also in the

vast and diffuse digestive system. Fundamental medical principles, such as hormone

action, distant physiologic regulation, and ductless secretion were once mysteries.

They now form the basis of basic medical diagnostics and therapeutics. This article

discusses and reviews the rich history that served as the foundation of modern medi-

cine, from the early descriptions of tumors, to the discovery of hormones and assays,

and how they resulted in the treatments available today.

EARLY DESCRIPTIONS OF THE GEP ENDOCRINE AXIS

Ancient physicians recognized the importance of certain glands in disease. The Chinese

described the role of the goiters in the thyroid, and the Egyptians saw the ovaries as

crucial to female reproduction.1,2But it was not until Galen that the concept of vital spirits

was developed in his studies of the pituitary in the second century.3 The description of

a

Department of Surgery, Surgical Oncology, Vanderbilt University, Medical Center, Nashville,TN, USAb Department of Endocrine Oncology, University Hospital, SE-751 85 Uppsala, Sweden* Corresponding author.E-mail address: kjell.oberg@medsci.uu.se

KEYWORDS

Gastroenteropancreatic endocrine axis Hormones Secretin Insulin Somatostatin Somatostatin analogs PRRT

Endocrinol Metab Clin N Am 39 (2010) 697711doi:10.1016/j.ecl.2010.09.002 endo.theclinics.com0889-8529/10/$ see front matter 2010 Elsevier Inc. All rights reserved.

mailto:kjell.oberg@medsci.uu.sehttp://dx.doi.org/10.1016/j.ecl.2010.09.002http://endo.theclinics.com/http://endo.theclinics.com/http://dx.doi.org/10.1016/j.ecl.2010.09.002mailto:kjell.oberg@medsci.uu.se

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glands took on greater meaning over the centuries as anatomists examined both ductal

and ductless organs, and secretions could find their way into other structures or directly

into the blood. In 1907, Sir Edward Sharpey-Schafer produced a model that unified the

various glandular organs into one comprehensive physiologic system.4

The principle of endocrine regulation was originated by Claude Bernard based on

the concepts of homeostasis.5 He used the term internal secretion in his descriptions

of the liver as an important component of homeostasis. These concepts matured

quickly with the classical endocrine organs, such as the adrenals, the thyroid, and

the lymphatics by the work of Thomas Addison, John Hunter, Theodor Kocher,

and Charles Edouard Brown Sequard.69 The descriptions of the GEP endocrine

system were more complicated and required the new technology of microscopy

before they could be investigated. Paul Langerhans as a medical student in 1869

then was able to describe small islands in the pancreas that would emerge as the islets

of Langerhans, and Nikolai Kulchitsky described the clear cells in the crypts of Lieber-

kuhn that now bear his name.10,11 While these were clearly important early discov-

eries, they were purely descriptive, as no function could be attributed to any of

these cells. The concept of a chemical messenger would have to wait until the turn

of the 20th century in one of the most famous experiments in medicine.

THE GUT AS AN ENDOCRINE ORGAN: SECRETIN

The dominant paradigm of gut physiology was the concept of nervism, developed first

by Karl Ludwig, then solidified by Ivan Pavlov and his famous dogs.1214 That evidence

stated that the nervous system was the regulator of bodily functions. In the specific

case of digestive secretion, Leon Popielski and E. Wertheimer tested the role of nervesin the regulation of pancreatic secretion in response to duodenal acidification by

aggressively denervating the abdominal organs in dogs and cats.15 In all instances,

they could not unlink the acid from the secretion, leading them both to conclude

that dedicated reflex nerves existed exclusively between the duodenum and the

pancreas. William Bayliss and Ernest Starling engaged the question of gastrointestinal

secretion by repeating the denervation experiments by Popieslki and Wertheimer, but

with a small modification.16

On Jan. 16, 1902, they concentrated the denervation to an isolated loop of jejunum,

carefully skeletonizing the intestines such that only the mesenteric vessels remained.17

Dilute hydrochloric acid was introduced into the bowel, and a steady flow of pancreaticjuice resulted, exactly as occurred in the duodenum. This simple experiment showed

that blood alone could carry a signal to start pancreatic secretion. As a follow-up,

they created an extract from scraped jejunal mucosa and injected it intravenously, again

causing a free flow of pancreatic fluid. They even showed that boiling did not destroy the

effect, and it could not be duplicated from distal ileal tissue. At that moment, Starling

declared, Then it must be a chemical reflex. Confident with this discovery, they

went on to present these data 6 days later at the Royal Society, calling their newly

discovered agent secretin. Before its publication in September, other scientists were

able to replicate these results and support grew for the chemical messenger theory.18

In fact, Pavlov himself repeated the experiment in late 1902, stating, Of course, they areright. It is clear that we did not take out an exclusive patent for the discovery of truth.19

These experiments led to the eventual development of and coining of the word hormone

(derived from the Greek to excite) by William Hardy to describe chemical messengers

as a class of physiologic regulators.20 In the following years, Starling recognized that the

gland secretion was in fact under dual control of both circulating chemicals and nerves.

Thus was the birth of the GEP neuroendocrine system.

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Other hormonal discoveries soon followed. Langley, Anderson, and Elliot were

studying adrenaline; Dale described histamine in 1910, and Edkins described

the potential existence of gastrin in 1905.2123 In the Croonian lecture to the Royal

College of Physicians, Starling not only cited those works, but also addressed the

potential of sex hormones and the antidiabetic effects of the pancreas.20 The

discovery of new GEP hormones would continue throughout the century and

continues today. The doctrine of hormone regulation would provide the platform for

further discoveries that not only influenced the understanding of the gut, but also

the development of techniques broadly used throughout science and medicine.

THE MOST FAMOUS HORMONE OF ALL: INSULIN

The discovery of secretin was a discovery of the fundamental physiologic pathway in

the GEP system. However, very few people died of secretin deficiency. Diabetes,

however, was a disease with a 100% mortality, and in children, it was a diagnosis

worse than cancer. Any new therapy would be accepted as an advance, but the

discovery of insulin was much more: for most, it was truly a miracle cure.24

The underlying mechanism was not well understood, but the symptoms were well

described. Since the Egyptians first recorded the sweet urine from diabetics, it was

known to be a disorder of sugars. Patients all developed the classical symptoms of

polydipsia, polyuria, fatigue, and frequently coma.2529 But there was no understanding

of the different types of diabetes. No one understood the difference between what is

now known as type 1 diabetes (autoimmune, or juvenile) versus type 2 diabetes (insulin

resistance, or adult-onset).30 The state-of-the-art therapy was championed by Dr

Frederick M. Allen, the leading authority at the time. From his studies at RockerfellerUniversity in New York, he developed a treatment of Draconian calorie restriction.3133

He recommended that diabetics only consume as much food as they could metabolize.

At the time that meant fasting until clearing of glucosuria. Then small amounts of food

were given until tolerance levels were achieved, which sometimes meant only a few

hundred calories a day. This left patients emaciated and lethargic, but could extend

their lives for a few months. Until the discovery of insulin, there was no other option;

prominent diabetologists, including Elliott Joslin of Boston, could only starve their

patients until they were living skeletons.34 Allen opened a clinic in New Jersey, and

the most prominent Americans went to him for treatment. It was understood, however,

that once the symptoms set in, that death was not far, especially in children.A young Canadian, army surgeon with farming roots, Frederick Banting, would find

himself at the Univeristy of Toronto, not because of his brilliance, but more because his

private practice was slow to establish.35 He took a lecturing position at the university

to supplement his income. In the fall of 1920, while preparing for a student lecture on

the pancreas, Banting noted that the islets of Langerhans are preserved in gallstone

pancreatitis, inspiring a short entry in his notebook:

Diabetes, ligate pancreatic ducts of dogs. Keep dogs alive till acini degenerateleaving Islets. Try to isolate the internal secretion of these to relieve glycosuria.

In May 1921, Banting, working with Professor J.J.R. Macleod, and a young medicalstudent, Charles Best, began work on the project. The experiment was straight

forward; Banting would open the abdomen of a dog, locate and ligate the pancreatic

duct, close the animal, and allow the exocrine tissue to die away. Several weeks later,

he would go back into the abdomen, perform a total pancreatectomy on the atrophied

gland and either graft it into another pancreatectomized dog, or try to develop an

extract of the internal secretion. Initially, it was Macleod who taught Banting how to

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perform the two-stage procedure. The standard method was to perform a near-total

pancreatectomy that did not cause diabetes. The pancreatic remnant was sutured

subcutaneously and the animal allowed to recover (note that the pancreas in a dog

is more diffuse than a human gland, which has a firm shape). In the second stage,

the remaining pancreas was removed, and the animal quickly became diabetic,

usually dying within a week. After establishing this technique, Banting went on to

the duct ligation. In a healthy animal, this procedure proved difficult; the duct was

small and hard to find, and it was easy to ligate pancreatic tissue instead of the duct.

Banting and Best used their allotted animals faster than they anticipated, but they

were able to procure stray dogs for their experiments, a common practice of the time.

Meanwhile, Macleod had left the university for summer vacation in Scotland. It was

a hot summer of work. The laboratories were hot, and the operating facilities smelled

of animal flesh. When they operated, their animals kept dying of infections, because

they could not keep the sweat or flies from entering the surgical field. When the dogs

were able to survive, they did not produce the desired results. When Banting went in

to recover the atrophied organ, he found a perfectly normal one. Several animals were

religated; several died in the process. Eventually a few dogs did atrophy, and their

organs were ground up and a liquid extraction prepared. They gave the extract to a dia-

betic depancreatized dog, and it lowered its blood sugars. Later experiments would

wake dogs from diabetic comas and dramatically lower blood sugar levels.36 Further

tests with extract from fetal cow, then adult cow pancreas would continue to be

successful, leading to the refinement of extract with the help of a new colleague, J.B.

Collip. They called this extract, isletin, which would later be known as insulin.37 Unfortu-

nately, as experiments succeeded, relationships failed. The country boy, Banting, saw

the intellectual professor, MacLeod, as stealing the credit. He saw Collip as takingover by producing better extract. In the beginning of 1922, at the first human test, Leo-

nard Thompson, a charity care boy with diabetes, down to 65 pounds, was given a crude

extract prepared by Banting and Best. It failed to lower his blood glucose. The failure was

crushing to Banting. Two weeks later, however, after Collip had optimized the extraction

process, another dose was given to Thompson; this time the results were truly spectac-

ular. The boys blood sugar dropped; his ketouria resolved, and he revived from a near

comatose state. Patients from all over North America descended upon Toronto. While

this stunning success should have led to celebration, it destroyed the dynamic of the

team, and paranoia set in. Eventually, Banting and Best received recognition for their

early work; Banting and MacLeod shared the Nobel Prize for Medicine in 1923.The miracle of insulin itself as a cure for deadly disease is enough drama alone, but

later in the century, insulin would find itself at the center of another race, to produce

the first recombinant hormone medication. It gave birth to huge pharmaceutical

companies such as Eli Lily, Novo Nordic, and Genentech.38 It provided Nobel prizes

to Frederick Sanger in 1958 (it was the first protein ever sequenced), Dorothy Crowfoot

Hodgkin in 1969 (it was the first protein whose structure was determined by radio-

graphic crystallography), and Rosalyn Sussman Yalow in 1977 (who developed the

first radioimmunoassay [RIA]against insulin).3943

TUMORS OF THE GEP: CARCINOID

Classical carcinomas of the small bowel were rare entities, but they had characteristic

pathologic features.44 However, a small series of patients with ileal tumors defied this

typical pathologic diagnosis. In 1867, Theodor Langhans first described a small, firm,

mushroom-shaped submucosal tumor from a 50-year-old woman who died of tuber-

culosis.45 He noted the unusual fact that it had sharp borders without any evidence of

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peritumoral invasion, with nests of rich, thick fibrous stroma. Twenty-one years later,

another series of patients was described by Otto Lubarsch, where ileal tumors were

found with tubercular growth patterns.46 He did note that diarrhea had been a promi-

nent symptom in one of the patients, consistent with the modern understanding of

these tumors. In Lubarschs review of the literature, he recognized that these tumors

were not consistent with carcinomas. Soon after, William Ransom described a case of

a 50-year-old woman with the symptoms of menorrhagia, abdominal masses, and

severe diarrhea with wheezing.47At the time, her symptoms were attributed to uterine

fibroids, but on autopsy, she was found to have several ileal nodules and hepatic

tumors. He noted that there was some malignant potential and termed them glan-

dular carcinomas.

The description of these tumors that has endured to modern times is attributed to

Siegfried Oberndorfer in 1907.48 His seminal paper first introduced the term karzinoide

to describe a series of patients with unusual tumors. His first case also involved

a patient who died of tuberculosis. At autopsy, he found four small tumors in the

submucosa of the ileum, with similar features to those previously described: nests

of cells with dense, fibrous connective disuse. The second case was a young woman

who died of typhoid fever; there were three small tumors in the ileum, all spaced far

away from each other. He had four more cases displaying similar findings; he

observed that there were multiple primary malignant tumors in the same organ. Obern-

dorfer concluded that these tumors were not true carcinoma; they grew slowly, had

sharp borders, and did not metastasize. He felt these odd tumors could not be

grouped with carcinoma of the small bowel, so he termed the carcinoma-like, hence

the term carcinoid. Unfortunately, Oberndorfers initial descriptions of carcinoid did

not encompass the true nature of the disease. It would be 22 yea rs later that he woulddescribe 36 more carcinoids of the appendix and small intestine.49 In those cases, he

revised his initial assessment to include the fact that the tumors were malignant and

had the potential to metastasize.

Further characterization of these tumors would rely on the new techniques being

developed in microscopy. First described in 1868, enterochromaffin cells of the gastric

mucosa were nothing more than a microscopic observation.50 In 1897, Nikolai Kulchit-

sky found similar staining cells in the crypts of Lieberkuhn.11,51,52 However, it was not

until 1914 that Pierre Masson applied silver stains to carcinoid tumors.53 In his first

description of an appendiceal carcinoid, he used saffron and trichrome stains to

observe a polarization of their secretory vesicles.54

From that, he deduced that thecarcinoid tumor was actually an endocrine neoplasm and that chromaffin cells were

the origin.55 Fourteen years later, Masson described enterochromaffin cells to be of

neural origin and stated that they could secrete substances. While the actual descrip-

tion of the carcinoid syndrome would not be documented until a few years later, the

microscopic cellular findings correlated well with clinic findings.

The collection of symptoms known as the carcinoid syndrome commonly includes

flushing, diarrhea, and edema. It was first formally described by Scholte, who docu-

mented an ileal carcinoid in a 47-year-old man who suffered from diarrhea, cyanosis,

cough, and lower extremity edema, who eventually died of heart failure and broncho-

pneumonia.56At autopsy, it was also noted that he had hard thickening of the tricuspidvalve and irregular endocardial thickening of the right atrium. This report was the first

documentation of carcinoid heart disease. Over the next 20 years, more cases were

published describing the syndrome with associated metastatic carcinoid. It was also

during this period, in 1948, that Rappoport first isolated and described serotonin.57 In

1954, Thorson and colleagues published the first series of patients presenting

with pulmonary stenosis, tricuspid insufficiency, peripheral vasomotor symptoms,

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bronchoconstriction, and cyanosis in association with malignant carcinoid tumor of the

small intestine with metastases to the liver.58 In the initial report, they presented seven

definite cases, four probable cases, and five with partial or not fully verified symptoms.

In the same year, Pernow and Waldenstrom added paroxysmal flushing as a key

component of this syndrome.59 Soon after, serotonin was isolated from enterochro-

maffin cells and eventually from an ileal carcinoid, proving that enterochromaffin cells

actually contained this bioactive amine. Lembeck confirmed in 1953 biochemically

the presence of serotonin in an ileal carcinoid tumor, thus concluding that human EC-

cells contained this bioactive ammine.60 In 1966, Anthony Pearse recognized that the

endocrine cells of the gut were linked together by a group of common cytochemical

characteristics, in particular, the uptake of 5-hydroxytryptophan and its decarboxyl-

ation to 5-HT.61 By 1968, these peptide hormone-producing cells, all of which derived

from the neural crest, were collectively entitled APUD (amine precursor uptake and

decarboxylation) cells, although more recently this acronym has been modified some-

what and is referred to as the diffuse neuroendocrine system (DNES).62 While Pearse

and others initially suggested that APUD cells were derived from neural crest cells, it

is now generally recognized that GEP APUD cells probably arise from endoderm. Le

Dourain and colleagues subsequently demonstrated that multipotency of neural crest

cells and proposed that enteric gangliogenesis by neural crest cells reflected the effects

of multiple growth factors of the glial-derived neurotrophic factor family.63,64

THE BIRTH OF THE DIFFUSE ENDOCRINE SYSTEM, ITS HORMONES, AND ITS DISEASES

This evolving concept of a diffuse endocrine system continued to mature and was firstformally described by Feyrter in 1938.65 By summing up decades of work on secretory

organs and cells, he recognized that the endocrine system consisted of traditional

compact epithelial organs as well as scattered cells either individually or in groups.

These cells could be seen not only in the pancreas, but also throughout the gut. He addi-

tionally recognized that these cells were connected within the neural network of the gut

wall. This structural relationship existed within the adrenal cortex and medulla, support-

ing a general and anatomically integrated model of the neuroendocrine system.

Famous syndromes would arise from the cells of the neuroendocrine system. The

adrenal glands were described in the 16th century, but it was not for another 300 years

that their importance was appreciated. In 1855, Addison described 12 patients withadrenal disorders, some who died of adrenal deficiency (Addison disease).7 In 1912,

Cushing described a patient with weight gain, muscle weakness, back pain, irregular

menstruations, a round face, hypertrichosis, hyperpigmentation, and extensive bleeding

with hypertension (Cushing syndrome).66 Eventually, this patient was recognized to

have hypercortism, and she was treated with a craniotomy and removal of the pituitary.

In 1927, Wilder described a case of insulin-secreting tumor, and later Whipple

described the clinical picture of hyperinsulinism.67,68 In 1948, glucagon was isolated

by Sutherland and de Duve, although some years previously Becker described prob-

ably the first glucagon-secreting tumor.69,70 The glucagonoma syndrome was well

documented by McGavran in 1966.71 In 1946, an ulcerogenic syndrome associatedwith a pancreatic islet cell tumor was described for the first time, and in 1955, Zollinger

and Ellison provided details of the syndrome that still carries their names.72 It was not

until 1964, however, that Gregory and Tracy isolated gastrin.73 In 1958, a description

was given of a diarrheogenic syndrome related to an endocrine tumor of the pancreas

by Verner and Morrison.74 This was many years before the hormone responsible vaso-

active intestinal polypeptide (VIP) was isolated.75 The identification of different inherited

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multiple endocrine adenomatoses syndrome was due to Wermer, Sipple and Williams,

and Pollock in 1954, 1961, and 1966 respectively.7678

Until 1960, most of the well-known clinical syndromes related to release of

substances from the gastro-pancreatic tract were described, although the exact

mediators were not delineated. Following the initial slow development in the recogni-

tion of GEP peptides/amines, there was an exponential rate of growth of discoveries in

relation to advances in protein chemistry that led to isolation and characterization of

more than 50 GEP peptides. An increased awareness of the actions of these

hormones, coupled with improved methods of detection, led to the recognition of

the role of these peptides in physiology and pathophysiology, and many tumor-asso-

ciated syndromes were predicted to overproduction of one or more GEP peptides/

amines. The late 1960s to early 1970s was the era of detection of a lot of new GEP

peptides/amines, particularly by work from Mutt and Jorpes from Stockholm. Viktor

Mutt was boiling tons of pig intestines and thereby could extract peptides, such as

VIP, GIP, PYY, and so forth.79 This was the golden era of GEP peptides.

SCIENCE CHANGES: INSULIN AND THE RIA

The disease known today as diabetes mellitus was well described in ancient times. The

symptoms of polyuria, polydipsia, and subsequent death were known to be associated

with sweet urine by ancient Egyptians, Indians, and Greeks. In fact, the term for diabetes

in the Chinese language is literally, sweet urine disease. The measurement of documen-

tation of diabetes has evolved over the centuries. Consistently, physicians made the diag-

nosis by tasting the urine. It became somewhat more objective when the ancient Chinese

and Indians tested a patients urine to see if it was sweet enough to attract ants. Bantingand Best, in their famousdogexperiments,were ableto measure blood glucose levelsand

urine glucose to nitrogen ratiosto documentdiabetes. However,a revolutionary technique

was developed that would change the way scientists could measure extremely small

quantities of biologically interesting molecules, all from insulin.

Insulin measurements are a relatively trivial technique by todays standards, but in

the early 20th century, normal insulin levels in the blood were not defined. The only

tools available at the time were biologic; an extract of tissue or serum was injected

into a depancreatized, adrenalectomized, or hypophysectomized animal, and the

drop in blood glucose was used as the outcome.80 This method had poor accuracy,

precision, reproducibility, and sensitivity. Moreover, it usually required large amountsof serum to get any type of effect. Other assays were developed involving rat dia-

phragm muscle or epididymal fat pads and their glucose uptake.81,82 However, in

addition to the previously mentioned problems, these tests were also influenced by

insulin-like molecules that could change blood glucose metabolism. These problems

were solved by the RIA.83

Rosalyn Yalow and Solomon Berson settled in the New York area and worked

together at the Brown Veterans Administration Hospital in the Radioisotope Unit:

Yalow the scientist, Berson the physician. They started their studies with 131I-labelled

insulin and its metabolism in diabetes. They were able to show that people with dia-

betes treated with insulin always produced anti-insulin antibodies. These antibodieswould be well characterized, but they would also be used as a tool. Yalow and Berson

recognized that this competitive binding of an unknown amount of unlabelled insulin

with a known amount of radiolabeled insulin to a known amount of antibody could

accurately measure the amount of insulin, even in a vast mixture of other molecules.

The discovery of RIA was published in 1960 and led to a Nobel Prize in 1977.43

More importantly, it provided the basis of measuring small quantities of other

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hormones. It supported earlier theories that there were two major types of diabetes,

one insulin-deficient (type 1 diabetes) and one insulin-resistant (type 2 diabetes).

Studies based on RIA also showed that insulin resistance was associated with obesity,

gestational diabetes, acromegaly, and Cushing disease.84,85 While confusing at first,

other insulin-like molecules eventually would be described (IGF-1 and IGF-2). RIA

also was used as an important tool to study membrane receptors, which previously

were difficult to detect and quantify. Eventually, this technique would be the standard

to measure proteins, peptides, and other molecules in all fields of medicine.

FROM BRAIN TO GUT: SOMATOSTATIN

The history of somatostatin left an indelible mark on the central and digestive nervous

systems. While its discovery was not as dramatic as insulin, the story of somatostatin

is tightly woven with insulin, and their paths cross throughout endocrine history. In its

own right, somatostatin has many powerful physiologic effects and is used by manycell types with diverse biologic effects.

The story of somatostatin begins in the brain, where growth hormone (GH) was an

important topic of research. It was well known that GH was expressed by pituitary and

had profound peripheral effects. What was unknown in the 1960s was how GH was

regulated. In 1964, GH-releasing hormone (GHRH) was isolated from the stalkmedian

eminences of sheep hypothalamus.86 During the column purification of GHRH,

another fraction contained a substance that had inhibitory effects on growth hormone

releasea GH-inhibiting factor (GIF). In 1968, Krulich and colleagues isolated from rat

hypothalamus a substance with an inhibiting action of the release of pituitary GH and

called it GH RIF.87

In the same year, Hellman and Lernmark reported on the presenceof a potent inhibitor of insulin secretion in extracts of pancreatic islets.88 Eventually,

GIF would be isolated and purified from 500,000 sheep hypothalami by Guillemin

and Brasseau using a new in vitro assay in 1973.89,90 As multiple groups competed

for its discovery and characterization, it went through many names, including GIF,

somatotropin release-inhibiting factor (SRIF), panhibin, and somatostatin. Shortly after

its discovery and characterization, the structure of somatostatin was solved and

allowed it to be purified and synthesized.91 Using RIA and immunohistochemistry

methods, it was shown that somatostatin-like immunoreactivity was heterogeneously

distributed in tissue of many animal species, vertebrate as well as in vertebrates.

The first somatostatin-producing neoplasm of the endocrine pancreas was describedin 1977 by Larsson and colleagues, and the clinical presentation included diabet es

mellitus, gallbladder disease, anemia, delayed gastric emptying, and loss of weight.92

Somatostatin inhibits the secretion of several gut hormones (eg, insulin and glucagon)

and digestive events, such as stomach acid and pancreatic fluid secretion. The

discovery of somatostatin and its effects would be rewarded with a Nobel Prize in

1977 to Roger Guillemin and Andrew Schally, the same year as Rosalyn Yalow .

It was in mid 1970s that the history of somatostatin mixed with that of insulin. 38 Up

until this time, insulin was purified from porcine pancreas, but injections were painful

and often associated with bad reactions. The race to produce a synthetic insulin

absorbed the time of multiple groups in the United States. Some groups chose toproduce it as a recombinant protein in genetically altered bacteria, but another group

chose a chemical route. Keiichi Itakura, Herbert Boyer, and Arthur Riggs set forth to

chemically construct a whole gene and implant it into a bacteria to produce a recombi-

nant human insulin. However, before they could tackle a gene the size of insulin, they

chose to test their technique on a much smaller protein, somatostatin. Itakura chemi-

cally synthesized a gene that would code for the 14 amino acid long peptide and implant

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Fig. 1. The historical development of the gastroenteropancreatic endocrine axis.

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it into Eshcerichia coli.93 The experiment worked. Unlike their competitors, who were

facing major public and political resistance to putting human genes into bacteria, Ita-

kura, Boyer, and Riggs saw no conflict in their chemical gene. This technology gave

birth to the pharmaceutical company Genentech. It was a short step to scaling up the

procedure to produce insulin. Thus, somatostatin was the first recombinant human

peptide ever synthesized in large quantities by bacterial recombination.

In 1978, Vale and Riviere reported on an octapeptide analog that displayed the full

biologic activity of somatostatin, and from 1980 to 1982, Bauer and colleagues at San-

doz synthesized an analog named octreotide.94,95 Shortly thereafter, other companies

and research institutes became interested in somatostatin analogs and produced

several other analogs, such as lanreotide and RC16O, and most recently SOM230

(Pasireotide by Novartis). Five somatostatin receptor subtypes (SSTR1-SSTR5) have

been identified by gene cloning techniques.96 These subtypes also differ in their binding

affinity to specific somatostatin analogs, an important characteristic relevant to imaging

and therapeutics. All somatostatin receptor subtypes are G-protein coupled receptors.

In 1982, Reubi and colleagues reported on the expression of somatostatin receptor

type 2 in neuroendocrine tumors (NETs).97,98 In 1983, the first somatostatin analogs

were used in clinical practice for treatment of severe clinical symptoms related to

NETs, such as carcinoid syndrome, the Verner Morrison syndrome, and glucagonoma

syndrome.99 Since then, the synthetic analog of somatostatin, octreotide (Sandosta-

tin), proved to be an excellent therapy to control the symptoms from NETs, and

convenient to administer (one injection every 4 weeks). Somatostatin receptor was

also a powerful target in NET diagnostics. In 1989, somatostatin receptor scintigraphy

was introduced by Krenning and his research group in Holland and later in the beginning

of 1990s, Krennings group introduced tumor targeted radioactive treatment (PRRT)with radiolabeled somatostatin analogs for treatment.100,101 In the beginning111

indium-labeled, later on 90yttrium, and finally 177lutetium-DOTA-octreotate were

applied in the treatment of various NETs.102105 Today therapy with somatostatin

analogs is the gold standard for patients with functioning tumors. Somatostatin scintig-

raphy is a working horse in the management of neuroendocrine tumors. It will soon be

replaced by positron emission tomography using 68gallium-DOTA-octreotate.106

From 1980 to 1990, new peptides were identified, which could be used as tumor

markers in GEP-NETs. The authors group reported on the expression of tachykinins

in carcinoid tumors in 1984.107 In 1986, OConnor and Deftos described the use of

chromogranin A as a general tumor marker in peptide-producing endocrineneoplasms.108 This marker is now the gold standard for diagnosis and follow-up of

different types of neuroendocrine tumors. Chromogranin A is a member of the chro-

mogranin family, stored in secretory granules of 80% of all NETs. The latest described

clinical syndrome related to GEP-NET was published from the authors group in

2004.109 It was a patient with a ghrelin-producing tumor of the gut. Ghrelin-producing

tumors have been published from other groups involving the pancreas and stomach.

Many NETs can ectopically produce other hormones such as ACTH, GRP, calcitonin,

HCG-a and PTH-RP. A summary is found in Fig. 1.

SUMMARY

For those with an interest in the GEP axis, its history is as compelling and fascinating

as the hormones themselves. When a patient complains of flushing and diarrhea,

those were the same complaints seen by Oberdorffer. When a young person with

newly diagnosed diabetes starts insulin, it is the same miracle treatment discovered

by Banting and Best. When a NET is treated with somatostatin analog, it is thanks

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to chemists and biologists that it can be injected just once a month. Over the decades,

GEP hormone research has been recognized at the highest levels, not only for its

effects on patients, but its effects on science. As long as there are still patients who

struggle with GEP diseases, there will still be more history to write.

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